Transcriptomic Analysis Reveals Cilostazol's Role in Ameliorating Cardiovascular Disease: Inhibition of Monocyte-to-macrophage Differentiation and Reduction of Endothelial Cell Reactive Oxygen Species Production

Overview

Journal Heliyon

Specialty Social Sciences

Date 2024 Apr 11

PMID 38601627

Authors

Chia-Ning Fan

Tsung-Neng Tsai

Xin-Jie Lu

Hsing-Fan Lai

Chun-Hua Wang

Yi-Lin Chiu

Affiliations

Soon will be listed here.

Abstract

Background: Cardiovascular diseases (CVDs) are the leading global cause of death, with atherosclerosis as the primary cause. Chronic inflammation, endothelial dysfunction, and the role of molecules like nitric oxide and reactive oxygen species are crucial in this context. Our previous research indicated that cilostazol and ginkgo biloba extract could enhance the ability of endothelial cells to dissolve blood clots, but the effects of cilostazol on monocytes remain unexplored.

Method: This study utilized peripheral blood mononuclear cells from 10 healthy donors, treated ex vivo with cilostazol. RNA-sequencing, over-representation analysis, xCell stromal cell analysis, and Gene Set Enrichment Analysis were employed to investigate the gene expression changes and biological pathways affected by cilostazol treatment.

Results: The study identified specific gene sets and pathways that were enriched or reduced in response to cilostazol treatment, providing insights into its effects on monocytes and potential therapeutic applications in CVD. The analysis also revealed the potential impact of cilostazol on the stromal cell compartment, further broadening our understanding of its multifaceted role.

Conclusion: The findings offer a nuanced understanding of the advantages and mechanisms of cilostazol in CVD, uncovering novel therapeutic targets and strategies to enhance the clinical application of cilostazol and contributing to the broader implications of this therapy in cardiovascular health.

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